Your search keyword '"FAMILIAL spastic paraplegia"' showing total 32 results

1. A pseudo‐homozygous missense variant and Alu‐mediated exon 5 deletion in FARS2 causing spastic paraplegia 77.

Author

Lin, Shu‐Huai, Xie, Jun‐Hao, Jiang, Jun‐Yi, Yan, Xin‐Yu, Hong, Chao‐Yin, Chen, Wan‐Jin, Wang, Ning, and Lin, Xiang

Subjects

*MISSENSE mutation, *SYMPTOMS, *NEURODEGENERATION, *PARAPLEGIA, *FAMILIAL spastic paraplegia, *SIBLINGS

Abstract

FARS2‐associated hereditary spastic paraplegia, later onset spastic paraplegia type 77, is a rarely neurodegenerative disease. Here, we reported two affected siblings in an autosomal recessive spastic paraplegia family with a pseudo‐homozygous missense variant and Alu‐mediated exon 5 deletion in FARS2. Both patients gradually developed altered gaits and weakness in both lower limbs. In our literature review, spastic paraplegia type 77 shows high heterogeneity in clinical manifestations. Our study broadens the scope of pathogenic mechanisms of SPG77 resulting from compound heterozygous mutations in FARS2 and provides strong evidence that deletion in FARS2 due to recombination event mediated by Alu element. [ABSTRACT FROM AUTHOR]

Published

2024

2. Characterization of a novel TFG variant causing autosomal recessive pure hereditary spastic paraplegia.

Author

Hsiao, Cheng‐Tsung, Tsai, Tzu‐Yun, Shen, Ting‐Yi, Tsai, Yu‐Shuen, Liao, Yi‐Chu, Lee, Yi‐Chung, and Tsai, Pei‐Chien

Subjects

*FAMILIAL spastic paraplegia, *RECESSIVE genes, *MUTANT proteins

Abstract

Objective: TFG mutations have previously been implicated in autosomal recessive hereditary spastic paraplegia (HSP), also known as SPG57. This study aimed to investigate the clinical and molecular features of TFG mutations in a Taiwanese HSP cohort. Methods: Genetic analysis of TFG was conducted in 242 unrelated Taiwanese HSP patients using a targeted resequencing panel covering the entire coding regions of TFG. Functional assays were performed using an in vitro cell model to assess the impact of TFG variants on protein function. Additionally, other representative TFG mutant proteins were examined to understand the broader implications of TFG mutations in HSP. Results: The study identified a novel homozygous TFG c.177A>C (p.(Lys59Asn)) variant in a family with adolescent‐onset, pure form HSP. Functional analysis revealed that the Lys59Asn TFG variant, similar to other HSP‐associated TFG mutants, exhibited a low affinity between TFG monomers and abnormal assembly of TFG homo‐oligomers. These structural alterations led to aberrant intracellular distribution, compromising TFG's protein secretion function and resulting in decreased cellular viability. Interpretation: These findings confirm that the homozygous TFG c.177A>C (p.(Lys59Asn)) variant is a novel cause of SPG57. The study expands our understanding of the clinical and mutational spectrum of TFG‐associated diseases, highlighting the functional defects associated with this specific TFG variant. Overall, this research contributes to the broader comprehension of the genetic and molecular mechanisms underlying HSP. [ABSTRACT FROM AUTHOR]

Published

2024

3. Late‐onset Krabbe disease presenting as spastic paraplegia – implications of GCase and CTSB/D.

Author

Mächtel, Rebecca, Dobert, Jan‐Philipp, Hehr, Ute, Weiss, Alexander, Kettwig, Matthias, Laugwitz, Lucia, Groeschel, Samuel, Schmidt, Manuel, Arnold, Philipp, Regensburger, Martin, and Zunke, Friederike

Subjects

*CATHEPSIN B, *CATHEPSIN D, *GAIT disorders, *PARAPLEGIA, *MISSENSE mutation, *FAMILIAL spastic paraplegia

Abstract

Objective: Krabbe disease (KD) is a multisystem neurodegenerative disorder with severe disability and premature death, mostly with an infancy/childhood onset. In rare cases of late‐onset phenotypes, symptoms are often milder and difficult to diagnose. We here present a translational approach combining diagnostic and biochemical analyses of a male patient with a progressive gait disorder starting at the age of 44 years, with a final diagnosis of late‐onset KD (LOKD). Methods: Additionally to cerebral MRI, protein structural analyses of the β‐galactocerebrosidase protein (GALC) were performed. Moreover, expression, lysosomal localization, and activities of β‐glucocerebrosidase (GCase), cathepsin B (CTSB), and cathepsin D (CTSD) were analyzed in leukocytes, fibroblasts, and lysosomes of fibroblasts. Results: Exome sequencing revealed biallelic likely pathogenic variants: GALC exons 11–17: 33 kb deletion; exon 4: missense variant (c.334A>G, p.Thr112Ala). We detected a reduced GALC activity in leukocytes and fibroblasts. While histological KD phenotypes were absent in fibroblasts, they showed a significantly decreased activities of GCase, CTSB, and CTSD in lysosomal fractions, while expression levels were unaffected. Interpretation: The presented LOKD case underlines the age‐dependent appearance of a mildly pathogenic GALC variant and its interplay with other lysosomal proteins. As GALC malfunction results in reduced ceramide levels, we assume this to be causative for the here described decrease in CTSB and CTSD activity, potentially leading to diminished GCase activity. Hence, we emphasize the importance of a functional interplay between the lysosomal enzymes GALC, CTSB, CTSD, and GCase, as well as between their substrates, and propose their conjoined contribution in KD pathology. [ABSTRACT FROM AUTHOR]

Published

2024

4. Homozygous variant in COQ7 causes autosomal recessive hereditary spastic paraplegia.

Author

Qiu, Yusen, Xiong, Ying, Wang, Lulu, Zhu, Min, Tan, Dandan, and Hong, Daojun

Subjects

*FAMILIAL spastic paraplegia, *RECESSIVE genes, *MOTOR neuron diseases, *GENETIC variation

Abstract

Biallelic mutations in the coenzyme Q7 (COQ7) encoding gene were recently identified as a genetic cause of distal hereditary motor neuropathy. Here, we explored the clinical, electrophysiological, pathological, and genetic characteristics of a Chinese patient with spastic paraplegia associated with recessive variants in COQ7. This patient carried a novel c.322C>A (p.Pro108Thr) homozygous variant. Sural biopsy revealed mild mixed axonal and demyelinating degeneration. Immunoblotting showed a significant decrease in the COQ7 protein level in the patient's fibroblasts. This study confirmed that COQ7 variant as a genetic cause of HSP, and further extended spastic paraplegia to the phenotypic spectrum of COQ7‐related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

5. Dystonia, spastic tetraplegia, and ataxia due to a novel mutation in the dynamin domain of OPA1.

Author

Shi, YuZhi, Zhang, Kang, Dong, GeHong, Pan, Hua, Chen, Bin, Wang, An, Niu, SongTao, Wang, XinGao, and Zhang, ZaiQiang

Subjects

*QUADRIPLEGIA, *ATAXIA, *GENETIC disorders, *BASAL metabolism, *DYNAMIN (Genetics), *OXIDATIVE phosphorylation, *MOVEMENT disorders, *FAMILIAL spastic paraplegia, *DELETION mutation

Abstract

Movement disorders manifest in various hereditary neurodegenerative diseases. We reported a young man who presented with progressive upper limb dystonia, spastic tetraplegia, and ataxia. Whole‐exome sequencing (WES) revealed a novel variant, c.2357A > G, in the dynamin domain of OPA1. No mtDNA deletion was detected in muscle by long‐range PCR. Atrophy and decreased glucose metabolism of the basal ganglia were discovered. Decreased mtDNA copy number, fragmented mitochondria, slightly impaired oxidative phosphorylation, and increased autophagy were detected in mutant fibroblasts. Evident oxidative phosphorylation impairment and mtDNA deletions were not involved in the pathogenicity of this mutation unlike mutations in the GTPase domain of OPA1. [ABSTRACT FROM AUTHOR]

Published

2024

6. A novel autosomal dominant ERLIN2 variant activates endoplasmic reticulum stress in a Chinese HSP family.

Author

Wang, Juan, Zhao, Rongjuan, Cao, Hanshuai, Yin, Zhaoxu, Ma, Jing, Xing, Yingming, Zhang, Wei, Chang, Xueli, and Guo, Junhong

Subjects

*ENDOPLASMIC reticulum, *FAMILIAL spastic paraplegia, *GENETIC variation, *HELA cells

Abstract

Objective: Hereditary spastic paraplegia (HSP) has been reported rarely because of a monoallelic variant in ERLIN2. The present study aimed at describing a novel autosomal dominant ERLIN2 pedigree in a Chinese family and exploring the possible mechanism of HSP caused by ERLIN2 variants. Methods: The proband and his family underwent a comprehensive medical history inquiry and neurological examinations. Whole‐exome sequencing was performed on the proband, and Sanger sequencing was performed on some family members. HeLa cell lines and mouse primary cortical neurons were used for immunofluorescence (IF) and reverse transcription‐PCR (RT‐PCR). Results: Seven patients were clinically diagnosed with pure spastic paraplegia in four consecutive generations with the autosomal dominant inheritance model. All patients presented juvenile‐adolescent onset and gradually worsening pure HSP phenotype. Whole‐exome sequencing of the proband and Sanger sequencing of all available family members identified a novel heterozygous c.212 T>C (p.V71A) variant in exon 8 of the ERLIN2 gene. The c.212 T>C demonstrated a high pathogenic effect score through functional prediction. RT‐PCR and IF analysis of overexpressed V71A revealed an altered ER morphology and increased XBP‐1S mRNA levels, suggesting the activation of ER stress. Overexpression of V71A in primary cultured cortical neurons promoted axon growth. Interpretation: The novel c.212 T>C heterozygous variant in human ERLIN2 caused pure HSP. Moreover, c.212 T>C heterozygous variant in ERLIN2 increased ER stress and affected axonal development. [ABSTRACT FROM AUTHOR]

Published

2023

7. Microdeletion in distal PLP1 enhancers causes hereditary spastic paraplegia 2.

Author

Zhou, Xun, Wang, Yige, He, Runcheng, Liu, Zhenhua, Xu, Qian, Guo, Jifeng, Yan, Xinxiang, Li, Jinchen, Tang, Beisha, Zeng, Sheng, and Sun, Qiying

Subjects

*FAMILIAL spastic paraplegia, *DNA copy number variations, *GENE enhancers, *MISSENSE mutation, *DEVELOPMENTAL delay

Abstract

Objectives: Hereditary spastic paraplegia (HSP) is a genetically heterogeneous disease caused by over 70 genes, with a significant number of patients still genetically unsolved. In this study, we recruited a suspected HSP family characterized by spasticity, developmental delay, ataxia and hypomyelination, and intended to reveal its molecular etiology by whole exome sequencing (WES) and long‐read sequencing (LRS) analyses. Methods: WES was performed on 13 individuals of the family to identify the causative mutations, including analyses of SNVs (single‐nucleotide variants) and CNVs (copy number variants). Accurate circular consensus (CCS) long‐read sequencing (LRS) was used to verify the findings of CNV analysis from WES. Results: SNVs analysis identified a missense variant c.195G>T (p.E65D) of MORF4L2 at Xq22.2 co‐segregating in this family from WES data. Further CNVs analysis revealed a microdeletion, which was adjacent to the MORF4L2 gene, also co‐segregating in this family. LRS verified this microdeletion and confirmed the deletion range (chrX: 103,690,507–103,715,018, hg38) with high resolution at nucleotide level accuracy. Interpretations: In this study, we identified an Xq22.2 microdeletion (about 24.5 kb), which contains distal enhancers of the PLP1 gene, as a likely cause of SPG2 in this family. The lack of distal enhancers may result in transcriptional repression of PLP1 in oligodendrocytes, potentially affecting its role in the maintenance of myelin, and causing SPG2 phenotype. This study has highlighted the importance of noncoding genomic alterations in the genetic etiology of SPG2. [ABSTRACT FROM AUTHOR]

Published

2023

8. Biallelic DDHD2 mutations in patients with adult‐onset complex hereditary spastic paraplegia.

Author

Chou, Ying‐Tsen, Hsu, Shao‐Lun, Tsai, Yu‐Shuen, Lu, Yi‐Jiun, Yu, Kai‐Wei, Wu, Hsiu‐Mei, Liao, Yi‐Chu, and Lee, Yi‐Chung

Subjects

*FAMILIAL spastic paraplegia, *PROTON magnetic resonance spectroscopy, *GENETIC mutation, *CEREBELLAR ataxia

Abstract

Objective: Hereditary spastic paraplegias (HSPs) are a group of inherited neurodegenerative disorders characterized by slowly progressive lower limb spasticity and weakness. HSP type 54 (SPG54) is autosomal recessively inherited and caused by mutations in the DDHD2 gene. This study investigated the clinical characteristics and molecular features of DDHD2 mutations in a cohort of Taiwanese patients with HSP. Methods: Mutational analysis of DDHD2 was performed for 242 unrelated Taiwanese patients with HSP. The clinical, neuroimaging, and genetic features of the patients with biallelic DDHD2 mutations were characterized. A cell‐based study was performed to assess the effects of the DDHD2 mutations on protein expression. Results: SPG54 was diagnosed in three patients. Among them, two patients carried compound heterozygous DDHD2 mutations, p.[R112Q];[Y606*] and p.[R112Q];[p.D660H], and the other one was homozygous for the DDHD2 p.R112Q mutation. DDHD2 p.Y606* is a novel mutation, whereas DDHD2 p.D660H and p.R112Q have been reported in the literature. All three patients manifested adult onset complex HSP with additional cerebellar ataxia, polyneuropathy, or cognitive impairment. Brain proton magnetic resonance spectroscopy revealed an abnormal lipid peak in thalamus of all three patients. In vitro studies demonstrated that all the three DDHD2 mutations were associated with a considerably lower DDHD2 protein level. Interpretation: SPG54 was detected in approximately 1.2% (3 of 242) of the Taiwanese HSP cohort. This study expands the known mutational spectrum of DDHD2, provides molecular evidence of the pathogenicity of the DDHD2 mutations, and underlines the importance of considering SPG54 as a potential diagnosis of adult‐onset HSP. [ABSTRACT FROM AUTHOR]

Published

2023

9. PLP1 gene mutations cause spastic paraplegia type 2 in three families.

Author

Yao, Li, Zhu, Zeyu, Zhang, Chao, Tian, Wotu, and Cao, Li

Subjects

*FAMILIAL spastic paraplegia, *SPASTIC paralysis, *GENETIC mutation, *PARAPLEGIA, *MUSCLE tone, *FECAL incontinence, *WHITE matter (Nerve tissue)

Abstract

Objective: Spastic paraplegia type 2 (SPG2) is an X‐linked recessive (XLR) form of hereditary spastic paraplegia (HSP) caused by mutations in proteolipid protein 1 (PLP1) gene. We described the clinical and genetic features of three unrelated families with PLP1 mutations and reviewed PLP1‐related cases worldwide to summarize the genotype–phenotype correlations. Methods: The three probands were 23, 26, and 27 years old, respectively, with progressively aggravated walking difficulty as well as lower limb spasticity. Detailed physical examination showed elevated muscle tone, hyperreflexia, and Babinski signs in lower limbs. Brain MRI examinations were investigated for all cases. PLP1 mutations were identified by whole exome sequencing, followed by Sanger sequencing, family co‐segregation, and phenotypic reevaluation. Results: A total of eight patients with SPG2 were identified in these three families. The probands additionally had cognitive impairment, urinary or fecal incontinence, ataxia, and white matter lesions (WML) in periventricular regions, with or without kinetic tremor. Three hemizygous mutations in PLP1 were identified, including c.453+159G>A, c.834A>T (p.*278C), and c.434G>A (p.W145*), of which c.834A>T was first associated with HSP. Interpretation: We identified three families with complicated SPG2 due to three PLP1 mutations. Our study supports the clinically inter‐and intra‐family heterogeneity of SPG2. The periventricular region WML and cognitive impairment are the most common characteristics. The kinetic tremor in upper limbs was observed in 2/3 families, suggesting the spectrum of PLP1‐related disorders is still expanding. [ABSTRACT FROM AUTHOR]

Published

2023

10. Clinical and genetic characterization of NIPA1 mutations in a Taiwanese cohort with hereditary spastic paraplegia.

Author

Fang, Shih‐Yu, Chou, Ying‐Tsen, Hsu, Kuo‐Chou, Hsu, Shao‐Lun, Yu, Kai‐Wei, Tsai, Yu‐Shuen, Liao, Yi‐Chu, Tsai, Pei‐Chien, and Lee, Yi‐Chung

Subjects

*FAMILIAL spastic paraplegia, *SCHOENLEIN-Henoch purpura, *GENETIC mutation, *PROTEIN expression, *PATERNAL age effect

Abstract

Objective: NIPA1 mutations have been implicated in hereditary spastic paraplegia (HSP) as the cause of spastic paraplegia type 6 (SPG6). The aim of this study was to investigate the clinical and genetic features of SPG6 in a Taiwanese HSP cohort. Methods: We screened 242 unrelated Taiwanese patients with HSP for NIPA1 mutations. The clinical features of patients with a NIPA1 mutation were analyzed. Minigene‐based splicing assay, RT‐PCR analysis on the patients' RNA, and cell‐based protein expression study were utilized to assess the effects of the mutations on splicing and protein expression. Results: Two patients were identified to carry a different heterozygous NIPA1 mutation. The two mutations, c.316G>A and c.316G>C, are located in the 3′ end of NIPA1 exon 3 near the exon–intron boundary and putatively lead to the same amino acid substitution, p.G106R. The patient harboring NIPA1 c.316G>A manifested spastic paraplegia, epilepsy and schizophrenia since age 17 years, whereas the individual carrying NIPA1 c.316G>C had pure HSP since age 12 years. We reviewed literature and found that epilepsy was present in multiple individuals with NIPA1 c.316G>A but none with NIPA1 c.316G>C. Functional studies demonstrated that both mutations did not affect splicing, but only the c.316G>A mutation was associated with a significantly reduced NIPA1 protein expression. Interpretation: SPG6 accounted for 0.8% of HSP cases in the Taiwanese cohort. The NIPA1 c.316G>A and c.316G>C mutations are associated with adolescent‐onset complex and pure form HSP, respectively. The different effects on protein expression of the two mutations may be associated with their phenotypic discrepancy. [ABSTRACT FROM AUTHOR]

Published

2023

11. Mobile digital gait analysis objectively measures progression in hereditary spastic paraplegia.

Author

Loris, Evelyn, Ollenschläger, Malte, Greinwalder, Teresa, Eskofier, Björn, Winkler, Jürgen, Gaßner, Heiko, and Regensburger, Martin

Subjects

*FAMILIAL spastic paraplegia, *WALKING speed

Abstract

Progressive spasticity and gait impairment is the functional hallmark of hereditary spastic paraplegia (HSP), but due to inter‐individual variability, longitudinal studies on its progression are scarce. We investigated the progression of gait deficits via mobile digital measurements in conjunction with clinical and patient‐reported outcome parameters. Our cohort included adult HSP patients (n = 55) with up to 77 months of follow‐up. Gait speed showed a significant association with SPRS progression. Changes in stride time and gait variability correlated to fear of falling and quality of life, providing evidence that gait parameters are meaningful measures of HSP progression. [ABSTRACT FROM AUTHOR]

Published

2023

12. Phenotypic continuum of NFU1‐related disorders.

Author

Kaiyrzhanov, Rauan, Zaki, Maha S., Lau, Tracy, Sen, Sambuddha, Azizimalamiri, Reza, Zamani, Mina, Sayin, Gözde Yeşil, Hilander, Taru, Efthymiou, Stephanie, Chelban, Viorica, Brown, Ruth, Thompson, Kyle, Scarano, Maria Irene, Ganesh, Jaya, Koneev, Kairgali, Gülaçar, Ismail Musab, Person, Richard, Sadykova, Dinara, Maidyrov, Yerdan, and Seifi, Tahereh

Subjects

*FAMILIAL spastic paraplegia, *PHENOTYPES, *LEUKOENCEPHALOPATHIES, *MISSENSE mutation, *WHITE matter (Nerve tissue)

Abstract

Bi‐allelic variants in Iron–Sulfur Cluster Scaffold (NFU1) have previously been associated with multiple mitochondrial dysfunctions syndrome 1 (MMDS1) characterized by early‐onset rapidly fatal leukoencephalopathy. We report 19 affected individuals from 10 independent families with ultra‐rare bi‐allelic NFU1 missense variants associated with a spectrum of early‐onset pure to complex hereditary spastic paraplegia (HSP) phenotype with a longer survival (16/19) on one end and neurodevelopmental delay with severe hypotonia (3/19) on the other. Reversible or irreversible neurological decompensation after a febrile illness was common in the cohort, and there were invariable white matter abnormalities on neuroimaging. The study suggests that MMDS1 and HSP could be the two ends of the NFU1‐related phenotypic continuum. [ABSTRACT FROM AUTHOR]

Published

2022

13. New phenotype of RTN2‐related spectrum: Complicated form of spastic paraplegia‐12.

Author

Tian, Wotu, Zheng, Haoran, Zhu, Zeyu, Zhang, Chao, Luan, Xinghua, and Cao, Li

Subjects

*FAMILIAL spastic paraplegia, *MUSCLE tone, *EPILEPSY, *PHENOTYPES, *ENDOPLASMIC reticulum, *WESTERN immunoblotting

Abstract

Objective: Spastic paraplegia‐12 (SPG12) is a subtype of hereditary spastic paraplegia caused by Reticulon‐2 (RTN2) mutations. We described the clinical and genetic features of three SPG12 patients, functionally explored the potential pathogenic mechanism of RTN2 mutations, and reviewed RTN2‐related cases worldwide. Methods: The three patients were 31, 36, and 50 years old, respectively, with chronic progressive lower limb spasticity and walking difficulty. Physical examination showed elevated muscle tone, hyperreflexia and Babinski signs in the lower limbs. Patients 1 and 3 additionally had visual, urinary, and/or coordination dysfunctions. Patient 2 also had epileptic seizures. RTN2 mutations were identified by whole‐exome sequencing, followed by Sanger sequencing, segregation analysis, and phenotypic reevaluation. Functional examination of identified mutations was further explored. Results: Three variants in RTN2 were identified in Patient 1 (c.103C>T, p.R35X), Patient 2 (c.230G>A, p.G77D), and Patient 3 (c.337C>A, p.P113T) with SPG, respectively. Western blotting revealed the p.R35X with smaller molecular weight than WT and other two missense mutants. Immunostaining showed the wild type colocalized with endoplasmic reticulum (ER) in vitro. p.R35X mutant diffusely distributes in the cytoplasm, losing colocalization with ER. p.G77D and p.P113T co‐localized with ER, which was abnormally aggregated in clumps. Interpretation: In this study, we identified three cases with complicated SPG12 due to three novel RTN2 mutations, respectively, presenting various phenotypes: classic SPG symptoms with (1) visual abnormalities and sphincter disturbances or (2) seizures. The phenotypic heterogeneity might arise from the abnormal subcellular localization of mutant Reticulon‐2 and improper ER morphogenesis, revealing the RTN2‐related spectrum is still expanding. [ABSTRACT FROM AUTHOR]

Published

2022

14. Novel CAPN1 missense variants in complex hereditary spastic paraplegia with early‐onset psychosis.

Author

Alecu, Julian E., Saffari, Afshin, Jumo, Hellen, Ziegler, Marvin, Strelko, Oleksandr, Brownstein, Catherine A., Gonzalez‐Heydrich, Joseph, Rodan, Lance H., Gorman, Mark P., Sahin, Mustafa, and Ebrahimi‐Fakhari, Darius

Subjects

*FAMILIAL spastic paraplegia, *MISSENSE mutation, *GENETIC variation, *NEUROGENIC bladder, *BLADDER diseases, *PSYCHOSES

Abstract

CAPN1‐associated hereditary spastic paraplegia (SPG76) is a rare and clinically heterogenous syndrome due to loss of calpain‐1 function. Here we illustrate a translational approach to the case of an 18‐year‐old patient who first presented with psychiatric symptoms followed by spastic gait, intention tremor, and neurogenic bladder dysfunction, consistent with a complex form of HSP. Exome sequencing showed compound‐heterozygous missense variants in CAPN1 (NM_001198868.2: c.1712A>G (p.Asn571Ser)/c.1991C>T (p.Ser664Leu)) and a previously reported heterozygous stop‐gain variant in RCL1. In silico analyses of the CAPN1 variants predicted a deleterious effect and in vitro functional studies confirmed reduced calpain‐1 activity and dysregulated downstream signaling. These findings support a diagnosis of SPG76 and highlight that the psychiatric symptoms can precede the motor symptoms in HSP. Our results also suggest that multiple genes can potentially contribute to complex neuropsychiatric diseases. [ABSTRACT FROM AUTHOR]

Published

2022

15. Characteristics of serum neurofilament light chain as a biomarker in hereditary spastic paraplegia type 4.

Author

Kessler, Christoph, Serna‐Higuita, Lina Maria, Wilke, Carlo, Rattay, Tim W., Hengel, Holger, Reichbauer, Jennifer, Stransky, Elke, Leyva‐Gutiérrez, Alejandra, Mengel, David, Synofzik, Matthis, Schöls, Ludger, Martus, Peter, and Schüle, Rebecca

Subjects

*FAMILIAL spastic paraplegia, *CYTOPLASMIC filaments, *BIOMARKERS, *PANEL analysis, *TREATMENT effectiveness

Abstract

Objective: While the anticipated rise of disease‐modifying therapies calls for reliable trial outcome parameters, fluid biomarkers are lacking in spastic paraplegia type 4 (SPG4), the most prevalent form of hereditary spastic paraplegia. We therefore investigated serum neurofilament light chain (sNfL) as a potential therapy response, diagnostic, monitoring, and prognostic biomarker in SPG4. Methods: We assessed sNfL levels in 93 patients with SPG4 and 60 healthy controls. The longitudinal study of sNfL levels in SPG4 patients covered a baseline, 1‐year follow‐up and 2‐year follow‐up visit. Results: Levels of sNfL were significantly increased in patients with genetically confirmed SPG4 compared to healthy controls matched in age and sex (p = 0.013, r = 0.2). Our cross‐sectional analysis revealed a greater difference in sNfL levels between patients and controls in younger ages with decreasing fold change of patient sNfL elevation at older ages. Over our observational period of 2 years, sNfL levels remained stable in SPG4 patients. Disease severity and progression did not correlate with sNfL levels. Interpretation: Our longitudinal data indicate a stable turnover of sNfL in manifest SPG4; therefore, sNfL levels are not suitable to monitor disease progression in SPG4. However, sNfL may be valuable as a therapy response biomarker, since its turnover could be modified by interventions. As the course of sNfL levels appears to be most dynamic around the onset of SPG4, the ability to detect a therapy response appears to be especially promising in younger patients, matching the need to initiate treatment in early disease stages. [ABSTRACT FROM AUTHOR]

Published

2022

16. Neurofilament light chain is a cerebrospinal fluid biomarker in hereditary spastic paraplegia.

Author

Kessler, Christoph, Serna‐Higuita, Lina M., Rattay, Tim W., Maetzler, Walter, Wurster, Isabel, Hayer, Stefanie, Wilke, Carlo, Hengel, Holger, Reichbauer, Jennifer, Armbruster, Marcel, Schöls, Ludger, Martus, Peter, and Schüle, Rebecca

Subjects

*FAMILIAL spastic paraplegia, *CEREBROSPINAL fluid, *CYTOPLASMIC filaments, *ENZYME-linked immunosorbent assay, *BIOMARKERS

Abstract

Objective: Despite the need for diagnostics and research, data on fluid biomarkers in hereditary spastic paraplegia (HSP) are scarce. We, therefore, explore Neurofilament light chain (NfL) levels in cerebrospinal fluid (CSF) of patients with hereditary spastic paraplegia and provide information on the influence of demographic factors. Methods: The study recruited 59 HSP cases (33 genetically confirmed) and 59 controls matched in age and sex. Neurofilament light chain levels were assessed by enzyme‐linked immunosorbent assay. The statistical analysis included the effects of age, sex, and genetic status (confirmed vs. not confirmed). Results: Levels of CSF NfL were significantly increased in patients with hereditary spastic paraplegia compared to controls (median 741 pg/mL vs. 387 pg/mL, p < 0.001). Age (1.4% annual increase) and male sex (81% increase) impacted CSF NfL levels in patients. The age‐dependent increase of CSF NfL levels was steeper in controls (2.6% annual increase). Thus, the CSF NfL ratio of patients and matched controls—expressing patients' fold increases in CSF NfL—declined considerably with age. Interpretation: CSF NfL is a reliable cross‐sectional biomarker in hereditary spastic paraplegia. Sex is a relevant factor to consider, as male patients have remarkably higher CSF NfL levels. While levels also increase with age, the gap between patients and controls is narrowing in older subjects. This indicates distinct temporal dynamics of CSF NfL in patients with hereditary spastic paraplegia, with a rise around phenotypic conversion and comparatively static levels afterward. [ABSTRACT FROM AUTHOR]

Published

2021

17. Genetic heterogeneity of neuronal intranuclear inclusion disease: What about the infantile variant?

Author

Sikora, Jakub, Jedlickova, Ivana, Pristoupilova, Anna, Stranecky, Viktor, and Honzik, Tomas

Subjects

*HYPERPERFUSION, *FAMILIAL spastic paraplegia, *MAGNETIC resonance imaging, *ANTERIOR pituitary gland, *NEUROLOGICAL disorders, *DORSAL root ganglia, *NEURAL crest

Abstract

Some of the key clinical, neuroimaging and (neuro)pathology characteristics that allow I ante-mortem i identification of jNIID and aNIID may not be useful to diagnose iNIID patients. Chen et al.1 have demonstrated lack of abnormal CGG expansions in the I NOTCH2NLC i gene among European juvenile and adult patients with neuronal intranuclear inclusion disease (jNIID and aNIID). IIs in non-neuronal CNS cell types have been unambiguously reported in only one patient (less than 5% of astrocytes contained IIs).8 The extent and distribution of CNS neuronal loss may be variable, however, cerebellar (cortical) atrophy is almost universally present in iNIID patients. [Extracted from the article]

Published

2021

18. Multimodal evaluation of an Italian family with a hereditary spastic paraplegia and POLR3A mutations.

Author

Ruggiero, Lucia, Iovino, Aniello, Dubbioso, Raffaele, Cocozza, Sirio, Trovato, Rosanna, Aruta, Francesco, Pontillo, Giuseppe, Barghigiani, Melissa, Brunetti, Arturo, Santorelli, Filippo Maria, Manganelli, Fiore, and Iodice, Rosa

Subjects

*FAMILIAL spastic paraplegia, *CERVICAL cord, *SPINAL cord, *GENETIC mutation

Abstract

We describe an Italian family with adult‐onset pure hereditary spastic paraplegia due to biallelic variants in POLR3A gene [c.1909 + 22G > A and c.3839dupT (p.M1280fs*20]. MRI showed a mild hyperintensity of superior cerebellar peduncles and cervical spinal cord atrophy. The neurophysiological metrics about intracortical excitability showed higher values of motor thresholds and a significant reduction of short interval intracortical inhibition (SICI) in the patient with a more severe phenotype. Our multimodal evaluation further expands the wide phenotypic spectrum associated with mutations in the POLR3A gene. An extensive genotype–phenotype correlation study is necessary to explain the role of the many new mutations on the function of protein. [ABSTRACT FROM AUTHOR]

Published

2020

19. Novel CAPN1 mutations extend the phenotypic heterogeneity in combined spastic paraplegia and ataxia.

Author

Lai, Lu‐Lu, Chen, Yi‐Jun, Li, Yun‐Lu, Lin, Xiao‐Hong, Wang, Meng‐Wen, Dong, En‐Lin, Wang, Ning, Chen, Wan‐Jin, and Lin, Xiang

Subjects

*FAMILIAL spastic paraplegia, *PARAPLEGIA, *CEREBELLAR ataxia, *ATAXIA, *GENETIC mutation, *MISSENSE mutation

Abstract

Objective: Recessive mutations in the CAPN1 gene have recently been identified in spastic paraplegia 76 (SPG76), a complex hereditary spastic paraplegia (HSP) that is combined with cerebellar ataxia, resulting in an ataxia‐spasticity disease spectrum. This study aims to assess the influence of CAPN1 variants on the occurrence of SPG76 and identify factors potentially contributing to phenotypic heterogeneity. Methods: We screened a cohort of 240 unrelated HSP families for variants in CAPN1 using high‐throughput sequencing analysis. We described in detail the clinical and genetic features of the SPG76 patients in our cohort and summarized all reported cases. Results: Six unreported CAPN1‐associated families containing eight patients with or without cerebellar ataxia were found in our cohort of HSP cases. These patients carried three previously reported homozygous truncating mutations (p.V64Gfs*103, c.759+1G>A, and p.R285*), and three additional novel compound heterozygous missense mutations (p.R481Q, p.P498L, and p.R618W). Lower limbs spasticity, hyperreflexia, and Babinski signs developed in about 94% of patients, with ataxia developing in 63% of cases. In total, 33 pathogenic mutations were distributed along the three reported functional domains of calpain‐1 protein, encoded by CAPN1, with no hotspot region. A comparison of gender distribution between the two groups indicated that female SPG76 patients were significantly more likely to present with complicated HSP than male patients (P = 0.015). Interpretation: Our study supports the clinically heterogeneous inter‐ and intra‐family variability of SPG76 patients, and demonstrates that gender and calpain‐1 linker structure may contribute to clinical heterogeneity in SPG76 cases. [ABSTRACT FROM AUTHOR]

Published

2020

20. Impaired proteasome activity and neurodegeneration with brain iron accumulation in FBXO7 defect.

Author

Correa‐Vela, Marta, Lupo, Vincenzo, Montpeyó, Marta, Sancho, Paula, Marcé‐Grau, Anna, Hernández‐Vara, Jorge, Darling, Alejandra, Jenkins, Alison, Fernández‐Rodríguez, Sandra, Tello, Cristina, Ramírez‐Jiménez, Laura, Pérez, Belén, Sánchez‐Montáñez, Ángel, Macaya, Alfons, Sobrido, María J., Martinez‐Vicente, Marta, Pérez‐Dueñas, Belén, and Espinós, Carmen

Subjects

*CEREBELLUM degeneration, *FAMILIAL spastic paraplegia, *NEURODEGENERATION, *PARKINSONIAN disorders, *PARAPLEGIA

Abstract

Abstact: FBXO7 is implicated in the ubiquitin–proteasome system and parkin‐mediated mitophagy. FBXO7defects cause a levodopa‐responsive parkinsonian‐pyramidal syndrome(PPS). Methods: We investigated the disease molecular bases in a child with PPS and brain iron accumulation. Results: A novel homozygous c.368C>G (p.S123*) FBXO7 mutation was identified in a child with spastic paraplegia, epilepsy, cerebellar degeneration, levodopa nonresponsive parkinsonism, and brain iron deposition. Patient's fibroblasts assays demonstrated an absence of FBXO7 RNA expression leading to impaired proteasome degradation and accumulation of poly‐ubiquitinated proteins. Conclusion: This novel FBXO7 phenotype associated with impaired proteasome activity overlaps with neurodegeneration with brain iron accumulation disorders. [ABSTRACT FROM AUTHOR]

Published

2020

21. Clinical characteristics of Taiwanese patients with Hereditary spastic paraplegia type 5.

Author

Chou, Cheng‐Ta, Soong, Bing‐Wen, Lin, Kon‐Ping, Tsai, Yu‐Shuen, Jih, Kang‐Yang, Liao, Yi‐Chu, and Lee, Yi‐Chung

Subjects

*FAMILIAL spastic paraplegia, *SINGLE nucleotide polymorphisms, *MICROSATELLITE repeats, *SPINAL cord

Abstract

Objectives: To investigate the clinical, electrophysiological, neuroimaging characteristics and genetic features of SPG5 in Taiwan. Methods: Mutational analysis of the coding regions of CYP7B1 was performed by utilizing targeted resequencing analysis of the 187 unrelated Taiwanese HSP patients. The diagnosis of SPG5 was ascertained by the presence of biallelic CYP7B1 mutations. The SPG5 patients received clinical, electrophysiological, and neuroimaging evaluations. Disease severity was assessed by using the Spastic Paraplegia Rating Scale (SPRS) and the disability score. Two microsatellite markers as well as 18 single‐nucleotide polymorphism (SNP) markers flanking CYP7B1 were genotyped to assess the founder effect of the CYP7B1 p.R112* mutation. Results: Nineteen SPG5 patients from 17 families were identified. They typically presented an insidious onset progressive spastic paraparesis with proprioception involvement beginning at age 8 to 40 years. Their MRIs often showed white matter abnormalities in bilateral occipito‐parietal regions, spinal cord atrophy, and mild cerebellar atrophy. Six different mutations in CYP7B1 were recognized, including three novel ones (p.N131Ifs*4, p.A295V, and p.L439R). CYP7B1 p.R112* was the most common mutation and present in 88.2% of the 17 SPG5 pedigrees. The patients with homozygous CYP7B1 p.R112* mutations had a milder clinical severity. Detailed haplotype analyses demonstrated a shared haplotype in the 25 individuals carrying at least one single allele of CYP7B1 p.R112*, suggesting a founder effect. Interpretation: This study delineates the distinct clinical and genetic features of SPG5 in Taiwan and provides useful information for the diagnosis and management of SPG5, especially in patients of Chinese descent. [ABSTRACT FROM AUTHOR]

Published

2020

22. A deep intronic splice variant advises reexamination of presumably dominant SPG7 Cases.

Author

Verdura, Edgard, Schlüter, Agatha, Fernández‐Eulate, Gorka, Ramos‐Martín, Raquel, Zulaica, Miren, Planas‐Serra, Laura, Ruiz, Montserrat, Fourcade, Stéphane, Casasnovas, Carlos, López de Munain, Adolfo, and Pujol, Aurora

Subjects

*FAMILIAL spastic paraplegia, *SCHOENLEIN-Henoch purpura, *WESTERN immunoblotting, *ANTISENSE DNA

Abstract

Objective: To identify causative mutations in a patient affected by ataxia and spastic paraplegia. Methods: Whole‐exome sequencing (WES) and whole‐genome sequencing (WGS) were performed using patient's DNA sample. RT‐PCR and cDNA Sanger sequencing were performed on RNA extracted from patient's fibroblasts, as well as western blot. Results: A novel missense variant in SPG7 (c.2195T> C; p.Leu732Pro) was first found by whole‐exome sequencing (WES), while the second, also unreported, deep intronic variant (c.286 + 853A>G) was identified by whole‐genome sequencing (WGS). RT‐PCR confirmed the in silico predictions showing that this variant activated a cryptic splice site, inducing the inclusion of a pseudoexon into the mRNA sequence, which encoded a premature stop codon. Western blot showed decreased SPG7 levels in patient's fibroblasts. Interpretation: Identification of a deep intronic variant in SPG7, which could only have been detected by performing WGS, led to a diagnosis in this HSP patient. This case challenges the notion of an autosomal dominant inheritance for SPG7, and illustrates the importance of performing WGS subsequently or alternatively to WES to find additional mutations, especially in patients carrying one variant in a gene causing a predominantly autosomal recessive disease. [ABSTRACT FROM AUTHOR]

Published

2020

23. Slowed vertical saccades as a hallmark of hereditary spastic paraplegia type 7.

Author

Milenkovic, Ivan, Klotz, Sigrid, Zulehner, Gudrun, Sycha, Thomas, and Wiest, Gerald

Subjects

*FAMILIAL spastic paraplegia, *PROGRESSIVE supranuclear palsy, *VESTIBULO-ocular reflex, *PARKINSONIAN disorders, *PARAPLEGIA

Abstract

Anecdotal oculomotor disturbances have been described in spastic paraplegia type 7 (SPG7). We investigated oculomotor and vestibular dysfunction in five patients with genetically verified SPG7. All five patients exhibited significantly slower velocities of vertical saccades compared to controls, but significantly faster than in progressive supranuclear palsy, with upward saccades being particularly affected. Horizontal saccades, cerebellar oculomotor markers, and vestibuloocular reflex seem to be variably affected. Thus, albeit subclinical in some cases, slowing of the vertical saccades may belong to the phenotype of SPG7 and may serve as a valuable biomarker for differentiation from spastic ataxias and atypical parkinsonism. [ABSTRACT FROM AUTHOR]

Published

2019

24. Hereditary spastic paraplegia and prominent sensorial involvement: think MAG mutations!

Author

Roubertie, Agathe, Charif, Majida, Meyer, Pierre, Manes, Gael, Meunier, Isabelle, Taieb, Guillaume, Junta Morales, Raul, Guichet, Agnès, Delettre, Cecile, Sarzi, Emmanuelle, Leboucq, Nicolas, Rivier, François, and Lenaers, Guy

Subjects

*FAMILIAL spastic paraplegia, *RECESSIVE genes, *MYELIN sheath, *INTELLECTUAL disabilities, *DEVELOPMENTAL delay, *PERIPHERAL neuropathy, *BRAIN imaging

Abstract

Homozygous mutations in MAG, encoding the myelin‐associated glycoprotein, a transmembrane component of the myelin sheath, have been associated with SPG 75 recessive spastic paraplegia. Here, we report the first patient with two compound heterozygous novel MAG mutations (p.A151V and p.S373R) and early developmental delay with a progressive complex phenotype characterized by spastic paraplegia, peripheral sensorimotor neuropathy, intellectual disability, and sensorial dysfunctions with severe optic atrophy and hearing involvement. Brain imaging showed progressive global cerebellar atrophy. We propose that complex hereditary spastic paraplegia, with axonal and demyelinating polyneuropathy, sensorial impairment and intellectual disability might suggest MAG mutations. [ABSTRACT FROM AUTHOR]

Published

2019

25. P5CS expression study in a new family with ALDH18A1‐associated hereditary spastic paraplegia SPG9.

Author

Magini, Pamela, Marco‐Marin, Clara, Escamilla‐Honrubia, Juan M., Martinelli, Diego, Dionisi-Vici, Carlo, Faravelli, Francesca, Forzano, Francesca, Seri, Marco, Rubio, Vicente, and Panza, Emanuele

Subjects

*FAMILIAL spastic paraplegia, *ETIOLOGY of diseases, *GENETIC mutation, *PROTEIN expression

Abstract

In 2015–2016, we and others reported ALDH18A1 mutations causing dominant (SPG9A) or recessive (SPG9B) spastic paraplegia. In vitro production of the ALDH18A1 product, Δ1‐pyrroline‐5‐carboxylate synthetase (P5CS), appeared necessary for cracking SPG9 disease‐causing mechanisms. We now describe a baculovirus–insect cell system that yields mgs of pure human P5CS and that has proven highly valuable with two novel P5CS mutations reported here in new SPG9B patients. We conclude that both mutations are disease‐causing, that SPG9B associates with partial P5CS deficiency and that it is clinically more severe than SPG9A, as reflected in onset age, disability, cognitive status, growth, and dysmorphic traits. [ABSTRACT FROM AUTHOR]

Published

2019

26. Mutation spectrum of Charcot‐Marie‐Tooth disease among the Han Chinese in Taiwan.

Author

Hsu, Yun‐Hsin, Lin, Kon‐Ping, Guo, Yuh‐Cherng, Tsai, Yu‐Shuen, Liao, Yi‐Chu, and Lee, Yi‐Chung

Subjects

*CHARCOT-Marie-Tooth disease, *FAMILIAL spastic paraplegia, *MICROSATELLITE repeats, *ULNAR nerve, *LEBER'S hereditary optic atrophy, *GENE frequency, *NEURAL conduction

Abstract

Objective: Charcot‐Marie‐Tooth disease (CMT) is a clinically and genetically heterogeneous group of inherited neuropathies. Mutations in more than 90 genes have been implicated in CMT; however, the mutational spectrum of CMT in Chinese population remains obscure. This study aims to provide a comprehensive overview of the frequency of mutations in Taiwanese patients with CMT and look for genotype‐phenotype correlations. Methods: Mutational analyses were performed on 427 unrelated Taiwanese patients with CMT by polymorphic microsatellite markers analysis or real‐time fluorescent PCR for PMP22 duplication, Sanger sequencing for GJB1 mutations, and targeted sequencing covering 124 genes causing or relevant to inherited neuropathies. We also correlated the genotypes with the phenotypic features, such as age at disease onset and ulnar motor nerve conduction velocity. Results: Pathogenic mutations were identified in 312 patients (73.1%; 312/427), including 208 patients with a PMP22 duplication, 40 patients with a GJB1 mutation, and 64 patients with a mutation in one of other 18 CMT genes. A confirmed molecular diagnosis was achieved in 84.4% (266/315) of the patients with demyelinating CMT and 41.1% (46/112) of the patients with axonal CMT. Mutations in MPZ, MFN2, or NEFL are the most frequent disease causes in patients with infantile‐onset CMT (≤2 years), while PMP22 duplications and mutations in GJB1, MFN2, or MPZ are the frequent causes among patients with childhood‐ or adolescence‐onset CMT (3–9 years). Interpretation: This study provides a genotype‐phenotype landscape of CMT in Taiwan and highlights the unique spectrum of CMT genes frequencies among patients of Chinese origin. [ABSTRACT FROM AUTHOR]

Published

2019

27. A novel CPT1C variant causes pure hereditary spastic paraplegia with benign clinical course.

Author

Hong, Daojun, Cong, Lu, Zhong, Shanshan, Liu, Ling, Xu, Yan, and Zhang, Jun

Subjects

*FAMILIAL spastic paraplegia, *FAMILIES, *GENES, *MESSENGER RNA

Abstract

Hereditary spastic paraplegia 73 (SPG73) was currently identified in only one family with variant in the neuronal isoform of carnitine palmitoyl‐transferase 1C (CPT1C) gene. We described a new family, in which affected individuals exhibited pure hereditary spastic paraplegia with benign clinical course. Exome sequencing revealed a novel nonsense variant in the CPT1C gene. The level of CPT1C mutant transcript significantly decreased compared to that of wild‐type transcript, and can be recovered after cycloheximide administration, which indicated that nonsense‐mediated mRNA decay was a mechanism that might be responsible for the phenotype. Our findings expanded the clinical and genetic spectrum of SPG73. [ABSTRACT FROM AUTHOR]

Published

2019

28. Serum neurofilament light chain is increased in hereditary spastic paraplegias.

Author

Wilke, Carlo, Rattay, Tim W., Hengel, Holger, Zimmermann, Milan, Brockmann, Kathrin, Schöls, Ludger, Kuhle, Jens, Schüle, Rebecca, and Synofzik, Matthis

Subjects

*BIOLOGICAL tags, *FAMILIAL spastic paraplegia, *NEURODEGENERATION, *DISEASE progression, *RANK correlation (Statistics)

Abstract

Abstract: Blood biomarkers are still largely missing in hereditary spastic paraplegias (HSPs). We here explored Neurofilament light chain (NfL) as a biomarker in HSP. Serum NfL was assessed in 96 HSP (63 genetically confirmed), 96 healthy control, and 33 ALS subjects by single molecule array (Simoa). Compared to controls, NfL was increased in HSP (P < 0.001), correlating with cross‐sectional disease progression (ρ = 0.28). Levels were lower than in ALS (P < 0.001), allowing to differentiate HSP from ALS (AUC = 0.91). Serum NfL might serve as a biomarker in HSP indicating neuronal damage and, if confirmed longitudinally, disease progression. It might also support differentiating HSP from ALS. [ABSTRACT FROM AUTHOR]

Published

2018

29. A novel mutation in KIF5A in a Malian family with spastic paraplegia and sensory loss.

Author

Guinto, Cheick O., Diarra, Salimata, Diallo, Salimata, Cissé, Lassana, Coulibaly, Thomas, Diallo, Seybou H., Taméga, Abdoulaye, Chen, Ke‐Lian, Schindler, Alice B., Bagayoko, Koumba, Simaga, Assiatou, Blackstone, Craig, Fischbeck, Kenneth H., and Landouré, Guida

Subjects

*FAMILIAL spastic paraplegia, *GENETIC mutation, *SENSORY disorders, *ATROPHY, *NUCLEOTIDE sequencing, *HOMOZYGOSITY

Abstract

Hereditary spastic paraplegias ( HSPs) are well-characterized disorders but rarely reported in Africa. We evaluated a Malian family in which three individuals had HSP and distal muscle atrophy and sensory loss. HSP panel testing identified a novel heterozygous missense mutation in KIF5A (c.1086G>C, p.Lys362Asn) that segregated with the disease ( SPG10). Lys362 is highly conserved across species and Lys362Asn is predicted to be damaging. This study shows that HSPs are present in sub-Saharan Africa, although likely underdiagnosed. Increasing efficiency and decreasing costs of DNA sequencing will make it more feasible to diagnose HSPs in developing countries. [ABSTRACT FROM AUTHOR]

Published

2017

30. Lysosomal abnormalities in hereditary spastic paraplegia types SPG15 and SPG11.

Author

Renvoisé, Benoît, Chang, Jaerak, Singh, Rajat, Yonekawa, Sayuri, FitzGibbon, Edmond J., Mankodi, Ami, Vanderver, Adeline, Schindler, Alice B., Toro, Camilo, Gahl, William A., Mahuran, Don J., Blackstone, Craig, and Pierson, Tyler Mark

Subjects

*LYSOSOMAL storage diseases, *FAMILIAL spastic paraplegia, *CORPUS callosum, *WHITE matter (Nerve tissue), *FIBROBLASTS, *PARKINSONIAN disorders, *DISEASE risk factors

Abstract

Objective Hereditary spastic paraplegias ( HSPs) are among the most genetically diverse inherited neurological disorders, with over 70 disease loci identified ( SPG1-71) to date. SPG15 and SPG11 are clinically similar, autosomal recessive disorders characterized by progressive spastic paraplegia along with thin corpus callosum, white matter abnormalities, cognitive impairment, and ophthalmologic abnormalities. Furthermore, both have been linked to early-onset parkinsonism. Methods We describe two new cases of SPG15 and investigate cellular changes in SPG15 and SPG11 patient-derived fibroblasts, seeking to identify shared pathogenic themes. Cells were evaluated for any abnormalities in cell division, DNA repair, endoplasmic reticulum, endosomes, and lysosomes. Results Fibroblasts prepared from patients with SPG15 have selective enlargement of LAMP1-positive structures, and they consistently exhibited abnormal lysosomal storage by electron microscopy. A similar enlargement of LAMP1-positive structures was also observed in cells from multiple SPG11 patients, though prominent abnormal lysosomal storage was not evident. The stabilities of the SPG15 protein spastizin/ ZFYVE26 and the SPG11 protein spatacsin were interdependent. Interpretation Emerging studies implicating these two proteins in interactions with the late endosomal/lysosomal adaptor protein complex AP-5 are consistent with shared abnormalities in lysosomes, supporting a converging mechanism for these two disorders. Recent work with Zfyve26−/− mice revealed a similar phenotype to human SPG15, and cells in these mice had endolysosomal abnormalities. SPG15 and SPG11 are particularly notable among HSPs because they can also present with juvenile parkinsonism, and this lysosomal trafficking or storage defect may be relevant for other forms of parkinsonism associated with lysosomal dysfunction. [ABSTRACT FROM AUTHOR]

Published

2014

31. The case of a 37‐year‐old male with trouble ambulating and incontinence.

Author

Bega, Danny

Subjects

*SERODIAGNOSIS, *CEREBROSPINAL fluid, *DIAPERS, *MALES, *FAMILIAL spastic paraplegia, *SPASTICITY, *NEUROMYELITIS optica

Abstract

Summary: A 37 year‐old previously healthy man from Jamaica presented with 2‐3 months of progressive trouble ambulating and incontinence. By 1 month prior to arrival he was wheelchair bound and unable to ambulate even with assistance. He started to wear a diaper for bladder and bowel incontinence. He also complained of painless numbness in his legs over the same period of time. His exam is notable for marked weakness and spasticity in his legs, with hyper‐reflexia and clonus. He has a sensory level at the level of the umbilicus. An MRI shows a longitudinally extensive T2 signal change throughout the thoracic cord. His cerebrospinal fluid is mildly inflammatory. His HTLV‐1 antibody test is reactive. [ABSTRACT FROM AUTHOR]

Published

2020

32. The case of a 51‐year‐old man with 15 years of progressive leg spasticity.

Author

Larson, Danielle N.

Subjects

*FAMILIAL spastic paraplegia, *URINARY urge incontinence, *SPASTICITY, *GENETIC testing

Abstract

The patient is a 51-year-old male with 15 years of progressive leg weakness and inability to walk. Initial genetic testing of limited known HSP genetic variants may not be sufficient to identify pathologic variants, and in these cases, more detailed genetic testing should be considered. 2 Patients presenting with an HSP phenotype must have spinal imaging to rule out intramedullary spinal cord pathology or dural AV fistula. [Extracted from the article]

Published

2021